Human polyomaviruses and cancer: an overview

José Carlos Mann Prado; Telma Alves Monezi; Aline Teixeira Amorim; Vanesca Lino; Andressa Paladino; Enrique Boccardo

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Autor(es):	José Carlos Mann Prado ^[1] ; Telma Alves Monezi ^[2] ; Aline Teixeira Amorim ^[3] ; Vanesca Lino ^[4] ; Andressa Paladino ^[5] ; Enrique Boccardo ^[6] Número total de Autores: 6
Afiliação do(s) autor(es):	^[1] Universidade de Sao Paulo. Instituto de Ciencias Biomedicas. Departamento de Microbiologia - Brasil ^[2] Universidade de Sao Paulo. Instituto de Ciencias Biomedicas. Departamento de Microbiologia - Brasil ^[3] Universidade de Sao Paulo. Instituto de Ciencias Biomedicas. Departamento de Microbiologia - Brasil ^[4] Universidade de Sao Paulo. Instituto de Ciencias Biomedicas. Departamento de Microbiologia - Brasil ^[5] Universidade de Sao Paulo. Instituto de Ciencias Biomedicas. Departamento de Microbiologia - Brasil ^[6] Universidade de Sao Paulo. Instituto de Ciencias Biomedicas. Departamento de Microbiologia - Brasil Número total de Afiliações: 6
Tipo de documento:	Artigo Científico
Fonte:	Clinics; v. 73, 2018-10-11.
Resumo
The name of the family Polyomaviridae, derives from the early observation that cells infected with murine polyomavirus induced multiple (poly) tumors (omas) in immunocompromised mice. Subsequent studies showed that many members of this family exhibit the capacity of mediating cell transformation and tumorigenesis in different experimental models. The transformation process mediated by these viruses is driven by viral pleiotropic regulatory proteins called T (tumor) antigens. Similar to other viral oncoproteins T antigens target cellular regulatory factors to favor cell proliferation, immune evasion and downregulation of apoptosis. The first two human polyomaviruses were isolated over 45 years ago. However, recent advances in the DNA sequencing technologies led to the rapid identification of additional twelve new polyomaviruses in different human samples. Many of these viruses establish chronic infections and have been associated with conditions in immunosuppressed individuals, particularly in organ transplant recipients. This has been associated to viral reactivation due to the immunosuppressant therapy applied to these patients. Four polyomaviruses namely, Merkel cell polyomavirus (MCPyV), Trichodysplasia spinulosa polyomavirus (TSPyV), John Cunningham Polyomavirus (JCPyV) and BK polyomavirus (BKPyV) have been associated with the development of specific malignant tumors. However, present evidence only supports the role of MCPyV as a carcinogen to humans. In the present review we present a summarized discussion on the current knowledge concerning the role of MCPyV, TSPyV, JCPyV and BKPyV in human cancers. (AU)

Processo FAPESP:	08/57889-1 - Instituto de Ciência e Tecnologia para o Estudo das Doenças Associadas ao Papilomavírus
Beneficiário:	Luisa Lina Villa
Modalidade de apoio:	Auxílio à Pesquisa - Temático

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